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翻译后的上游区域的快速降解表明翻译起始过程效率低下。

The rapid degradation of translated upstream regions points to an inefficient translation initiation process.

作者信息

Tress Michael L

机构信息

Bioinformatics Unit, Spanish National Cancer Research Centre (CNIO), 28029 Madrid, Spain.

出版信息

bioRxiv. 2024 Nov 26:2024.11.25.625198. doi: 10.1101/2024.11.25.625198.

Abstract

Large-scale experimental analyses find ever more abundant evidence of translation from start codons upstream of the canonical start site. This translation either generates entirely new proteins (from novel upstream open reading frames) or produces isoforms with extended N-terminals when the novel start codon is in frame Most extended N-terminals are likely to just add a disordered region to the canonical protein isoform, but some may also block the recognition of the signal peptide causing the isoform to accumulate in the incorrect cellular compartment. This analysis finds evidence that upstream translations that would interfere with signal peptides are detected in expected quantities in ribosome profiling experiments, but that the equivalent N-terminally extended protein isoforms are significantly reduced in multiple proteomics experiments. This suggests that these isoforms are likely to be degraded shortly after translation by the ubiquitination pathway, thus preventing the build up of potentially harmful proteins with hydrophobic regions in the cytoplasm. In addition, this is further evidence that most of the transcripts translated from upstream start sites are the result of an inefficient translation initiation process. This has implications for the annotation of proteins given the huge numbers of upstream translations that are being detected in large-scale experiments.

摘要

大规模实验分析发现,越来越多的证据表明,在标准起始位点上游的起始密码子处存在翻译现象。这种翻译要么产生全新的蛋白质(来自新的上游开放阅读框),要么当新的起始密码子处于读框内时,产生具有延长N端的异构体。大多数延长的N端可能只是在标准蛋白质异构体上添加一个无序区域,但有些也可能会阻碍信号肽的识别,导致异构体在错误的细胞区室中积累。该分析发现,在核糖体谱实验中,预期数量的会干扰信号肽的上游翻译被检测到,但在多个蛋白质组学实验中,等效的N端延长蛋白质异构体显著减少。这表明这些异构体可能在翻译后不久就被泛素化途径降解,从而防止在细胞质中积累具有疏水区域的潜在有害蛋白质。此外,这进一步证明,从上游起始位点翻译的大多数转录本是低效翻译起始过程的结果。鉴于在大规模实验中检测到大量的上游翻译,这对蛋白质注释具有重要意义。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/dc88/11623489/9f4aab7f2b2e/nihpp-2024.11.25.625198v1-f0001.jpg

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